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Acrylonitrile interaction with testicular DNA in rats

โœ Scribed by Ahmed, Ahmed E. ;Abdel-Rahman, Sherif Z. ;Nour Deen, Amr M. -Al


Book ID
102875636
Publisher
John Wiley and Sons
Year
1992
Tongue
English
Weight
727 KB
Volume
7
Category
Article
ISSN
0887-2082

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โœฆ Synopsis


In the present study we report the in vivo interaction of acrylonitrile (VCN) with testicular tissue in rats. Covalent binding of radioactivity to testicular tissue DNA was examined for a period of 72 hr after a single oral dose (46.5 mg/kg) of [2,3-14C] VCN. Maximal covalent binding was observed at 0.5 hr (8.9 pmol VCN equivalenVmo1 nucleotide). Binding decreased gradually thereafter but was still detected (2.5 pmol VCN equivalent/mol nucleotide) at 72 hr following VCN administration. Further, we examined the effects of VCN on DNA synthesis and repair in the testes of rats following a single oral dose (46.5 mg/kg) of VCN to clarify the impact of the covalent binding observed on the testicular genetic material. A significant decrease in DNA synthesis (80% of control) was observed at 0.5 hr after treatment. At 24 hr following acrylonitrile administration, testicular DNA synthesis was severely inhibited (38% of control). Testicular DNA repair was increased 1.5-fold at 0.5 hr and more than 3.3-fold at 24 hr following treatment with VCN. These results suggest that VCN can act as a multipotent genotoxic agent by alkylating DNA in testicular tissue and may affect the male reproductive function by interfering with testicular DNA synthesis and repair processes.


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Molecular interaction of [2,3-14C] acryl
โœ Abdel-Rahman, Sherif Z. ;Nouraldeen, Amr M. ;Ahmed, Ahmed E. ๐Ÿ“‚ Article ๐Ÿ“… 1994 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 760 KB

## Abstract Acrylonitrile (VCN) is used extensively in polymer industries, and is known to induce gastric cancer following oral administration, A paucity of information exists regarding the mechanism(s) by which acrylonitrile induces gastric neoplasia. The time course for uptake of radioactivity by